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Activated lymphocytes as a metabolic model for carcinogenesis

机译:活化的淋巴细胞作为致癌作用的代谢模型

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Metabolic reprogramming is a key event in tumorigenesis to support cell growth, and cancer cells frequently become both highly glycolytic and glutamine dependent. Similarly, T lymphocytes (T cells) modify their metabolism after activation by foreign antigens to shift from an energetically efficient oxidative metabolism to a highly glycolytic and glutamine-dependent metabolic program. This metabolic transition enables T cell growth, proliferation, and differentiation. In both activated T cells and cancer cells metabolic reprogramming is achieved by similar mechanisms and offers similar survival and cell growth advantages. Activated T cells thus present a useful model with which to study the development of tumor metabolism. Here, we review the metabolic similarities and distinctions between activated T cells and cancer cells, and discuss both the common signaling pathways and master metabolic regulators that lead to metabolic rewiring. Ultimately, understanding how and why T cells adopt a cancer cell-like metabolic profile may identify new therapeutic strategies to selectively target tumor metabolism or inflammatory immune responses.
机译:代谢重编程是肿瘤发生中支持细胞生长的关键事件,癌细胞经常变得高度糖酵解和谷氨酰胺依赖性。同样,T淋巴细胞(T细胞)在被外源抗原激活后会改变其代谢,从而从能量有效的氧化代谢转变为高度糖酵解和谷氨酰胺依赖性的代谢程序。这种代谢转变使T细胞能够生长,增殖和分化。在活化的T细胞和癌细胞中,代谢重编程都是通过相似的机制实现的,并提供相似的生存和细胞生长优势。因此,活化的T细胞呈现出有用的模型,可用来研究肿瘤代谢的发展。在这里,我们审查了活化的T细胞和癌细胞之间的代谢相似性和区别,并讨论了导致代谢重新连接的常见信号传导途径和主要的代谢调节剂。最终,了解T细胞如何以及为何采用癌细胞样的代谢模式可能会确定新的治疗策略,以选择性地靶向肿瘤代谢或炎症性免疫反应。

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